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DNA Methylation Profile of the SREBF2 Gene in Human Fetal Aortas. | LitMetric

AI Article Synopsis

  • Research indicates that maternal cholesterol levels during pregnancy may increase the risk of atherosclerotic disease in their offspring, though the specific mechanisms are still unclear.
  • A study analyzed fetal aorta samples from aborted fetuses of mothers with normal and high cholesterol, finding significant DNA methylation changes in the SREBF2 gene in those from hypercholesterolemic mothers.
  • The results suggest a need for improved cardiovascular prevention programs for children of mothers with high cholesterol and highlight the importance of further investigating the epigenetic factors related to this issue.

Article Abstract

Increasing evidence suggests that maternal cholesterol represents an important risk factor for atherosclerotic disease in offspring already during pregnancy, although the underlying mechanisms have not yet been elucidated. Eighteen human fetal aorta samples were collected from the spontaneously aborted fetuses of normal cholesterolemic and hypercholesterolemic mothers. Maternal total cholesterol levels were assessed during hospitalization. DNA methylation profiling of the whole SREBF2 gene CpG island was performed (p value <0.05). The Mann-Whitney U test was used for comparison between the 2 groups. For the first time, our study revealed that in fetal aortas obtained from hypercholesterolemic mothers, the SREBF2 gene shows 4 significant differentially hypermethylated sites in the 5'UTR-CpG island. This finding indicates that more effective long-term primary cardiovascular prevention programs need to be designed for the offspring of mothers with hypercholesterolemia. Further studies should be conducted to clarify the epigenetic mechanisms underlying the association between early atherogenesis and maternal hypercholesterolemia during pregnancy.

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Source
http://dx.doi.org/10.1159/000518513DOI Listing

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